US2390335A - Method of preparing hydroxy derivatives of aliphatic acids and new compounds produced thereby - Google Patents

Method of preparing hydroxy derivatives of aliphatic acids and new compounds produced thereby Download PDF

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US2390335A
US2390335A US405408A US40540841A US2390335A US 2390335 A US2390335 A US 2390335A US 405408 A US405408 A US 405408A US 40540841 A US40540841 A US 40540841A US 2390335 A US2390335 A US 2390335A
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hydroxy
acid
crotonic acid
new compounds
compounds produced
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US405408A
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Harry H Sobotka
Martin I Rubin
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Mount Sinai Hospital Research Foundation Inc
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Mount Sinai Hospital Research Foundation Inc
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D315/00Heterocyclic compounds containing rings having one oxygen atom as the only ring hetero atom according to more than one of groups C07D303/00 - C07D313/00
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C59/00Compounds having carboxyl groups bound to acyclic carbon atoms and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
    • C07C59/40Unsaturated compounds
    • C07C59/42Unsaturated compounds containing hydroxy or O-metal groups

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  • the present invention relates to a method of preparing hydroxy derivatives of 11-13 unsaturated aliphatic acids and to certain new compounds produced thereby having utility in the synthesis of various intermediates which have importance in the synthesis of therapeutic compounds, e. g.. vitamin A and various other carotenoids.
  • the invention is based on our discovery that when an vac-,8 unsaturated aliphatic acid, or its ester or similar derivative. is treated with selenous acid, HzSeOs, or selenium dioxide, S802, under appropriate conditions as illustrated hereinafter, a methyl group forming the end of the aliphatic chain is oxidized to the group, CH2OH.
  • the resulting 7 hydroxy acid may be obtained as such or as its acyl (e. g., acetyl) derivative or as a lactone.
  • This method is of particular importance in preparing hydroxy derivatives of the normal and branched-chain unsaturated acids, such as crotonic acid and fi-methylcrotonic acid (dimethyl acrylic acid).
  • the oxidation may be performed without any solvent or in the presence of a solvent such as ethyl alcohol, dioxane or acetic anhydride.
  • a solvent such as ethyl alcohol, dioxane or acetic anhydride.
  • an acetoxy derivative is formed from which the corresponding hydroxy derivative is obtained by alcoholysis by means of sulfuric acid in ethyl alcohol or by use of sodium methylate.
  • Example I Crotonic acid ethyl ester (ethyl crotonate) was dissolved in 5 parts of dioXane and refluxed for 2 hours with of its weight of selenous acid with stirring. After complete disappearance of white selenous acid, the solid selenium was fil tered off and the solvent was removed under reduced pressure from the reaction mixture. The precipitated residue was then dissolved in ether and dried. The ether and unreacted starting material was removed by distillation and the lactone of -hydroxy crotonic acid was obtained by distillation in vacuo, boiling at 85 to 88 C. at 9 mm. pressure.
  • Example II 50 grams of the ethyl ester of dimethyl acrylic acid was dissolved in 200 cc. of acetic anhydride. This solution was heated to boiling, and during continuous stirring 25 grams of selenous dioxide were added over a period of one hour. After the addition, the solution was refluxed for an additional 2 hours. The precipitated selenium was filtered from the cooled solution. and the filtrate was thrown into 3% times its own volume of water. A reddish oil precipitated and was separated from the aqueous layer. The resulting oil precipitate amounting to 40 grams was shaken with 18 grams of sodium carbonate dissolved in 120 cc. of water.
  • Example III 50 grams of dimethyl acrylic acid ethyl ester were heated under reflux in an oil bath kept at C. and 25 grams of SeOz dissolved in 25 cc. of ethanol added dropwise over a period of 2 to 2%. hours. Heating and stirring was continued for one more hour. The solution was cooled and filtered from the precipitated selenium. The filtrate was diluted with 1 /2 times its volume of water. The final product obtained by distillation in vacuo is 'y-hydroxy fl-methyl crotonic acid ethyl ester of the same properties as the end product of Example II.
  • esters or similar derivatives of the 11,,8 unsaturated aliphatic acids are responsive to the indicated reactions, itwill be understood that the term similar derivatives is intended to include the corresponding anhydrides, acyl halogenides and nitriles, and that where in the claims the method is described as applied to the acids and their esters, the term esters is intended to include these similar derivatives.
  • the process for preparing 'y-hydroxy derivatives of normal and branched-chain oc-fl unsaturated aliphatic acid alkyl esters, which derivatives are characterized by the presence of an hydroxyl group in a methyl group attached to the c-carbon atom which comprises reacting a member of the group consisting of the normal and branched-chain oc-fl unsaturated aliphatic acid alkyl esters having a methyl group attached to the B-carbon atom, with selenous acid in the presence of a solvent.
  • R represents a radical selected from the group consisting of the acetoxy and hydroxyl groups
  • X represents a radical selected from the group consisting of hydrogen and an alkyl group

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  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)

Description

Patented Dec. 4, 1945 METHOD OF PREPARING HYDROXY DERIV- ATIVES F AL PHATIC ACIDS AND NEW COMPOUNDS PRODUCED THEREBY Harry H. Sobotka and Martin I. Rubin, New York,
N. Y., assignors to Mount Sinai Hospital Research Foundat on. Inc., a membership corporation of New York No Drawing. Application August 4, 1941, Serial No. 405,408
10 Claims.
The present invention relates to a method of preparing hydroxy derivatives of 11-13 unsaturated aliphatic acids and to certain new compounds produced thereby having utility in the synthesis of various intermediates which have importance in the synthesis of therapeutic compounds, e. g.. vitamin A and various other carotenoids.
The invention is based on our discovery that when an vac-,8 unsaturated aliphatic acid, or its ester or similar derivative. is treated with selenous acid, HzSeOs, or selenium dioxide, S802, under appropriate conditions as illustrated hereinafter, a methyl group forming the end of the aliphatic chain is oxidized to the group, CH2OH. The resulting 7 hydroxy acid may be obtained as such or as its acyl (e. g., acetyl) derivative or as a lactone. This method is of particular importance in preparing hydroxy derivatives of the normal and branched-chain unsaturated acids, such as crotonic acid and fi-methylcrotonic acid (dimethyl acrylic acid). The oxidation may be performed without any solvent or in the presence of a solvent such as ethyl alcohol, dioxane or acetic anhydride. When the lastnamed compound is used an acetoxy derivative is formed from which the corresponding hydroxy derivative is obtained by alcoholysis by means of sulfuric acid in ethyl alcohol or by use of sodium methylate.
Example I Crotonic acid ethyl ester (ethyl crotonate) was dissolved in 5 parts of dioXane and refluxed for 2 hours with of its weight of selenous acid with stirring. After complete disappearance of white selenous acid, the solid selenium was fil tered off and the solvent was removed under reduced pressure from the reaction mixture. The precipitated residue was then dissolved in ether and dried. The ether and unreacted starting material was removed by distillation and the lactone of -hydroxy crotonic acid was obtained by distillation in vacuo, boiling at 85 to 88 C. at 9 mm. pressure. This compound has the structural formula ([lHz-CH=CHCO Example II 50 grams of the ethyl ester of dimethyl acrylic acid was dissolved in 200 cc. of acetic anhydride. This solution was heated to boiling, and during continuous stirring 25 grams of selenous dioxide were added over a period of one hour. After the addition, the solution was refluxed for an additional 2 hours. The precipitated selenium was filtered from the cooled solution. and the filtrate was thrown into 3% times its own volume of water. A reddish oil precipitated and was separated from the aqueous layer. The resulting oil precipitate amounting to 40 grams was shaken with 18 grams of sodium carbonate dissolved in 120 cc. of water. The product, now the top layer, was separated from the aqueous portion. The aqueous layer was extracted once with ether and the ether extract combined with the main fraction. The combined extracts were washed with water, dried, freed from ether, and the residue was rectified twice under reduced pressure. The fraction boiling between 88 and 90 C. under 3-5 mm. pressure consisted of the 'y-acetoxy-B-methyl crotonic acid ethyl ester, refractive index N 1.4524. This compound has the formula CH3.CO.OCH2.C(CH3) =CH.COOE.t
The acetyl group was subsequently removed by alcoholysis with sulfuric acid, and the resulting 'y-hydroxy-,6-methyl crotonic acid ethyl ester was obtained as a colorless liquid of boiling point 92--94 C. under a pressure of {it-4 mm. of mercury, having a refractive index N11 =L4670 and a formula of HOCI-I2.C(CH3) :CHCOOEt This substance was further characterized by its 3', 5-dinitrobenzoyl-derivative of melting point 91 C.
Example III 50 grams of dimethyl acrylic acid ethyl ester were heated under reflux in an oil bath kept at C. and 25 grams of SeOz dissolved in 25 cc. of ethanol added dropwise over a period of 2 to 2%. hours. Heating and stirring was continued for one more hour. The solution was cooled and filtered from the precipitated selenium. The filtrate was diluted with 1 /2 times its volume of water. The final product obtained by distillation in vacuo is 'y-hydroxy fl-methyl crotonic acid ethyl ester of the same properties as the end product of Example II.
Both from the acetoxy ester and from the free hydroxy ester, there was obtained by hydrolysis with aqueous alkali -hydroxy-B-methyl crotonic acid of meltin point 108-109.5 0., having the formula HOCI-I2.C(CH3) :CHCOOH The method above disclosed permits the preparation of many 7 hydroxy unsaturated aliphatic acid derivatives having importance in organic synthesis as well as for other purposes. Among these compounds may be mentioned y-hydroxys-methyl crotonic acid and its alkyl esters, the existence of which was hitherto unknown. These compounds may be easily converted into the corresponding -bromo-p-methyl crotonic acid or its alkyl ester, as the case may be, by the action of PBrs as will be illustrated in the following example of a procedure that we have emplayed in producing 'ybromo-methyl crotonic acid ethyl ester.
Following a procedure similar to that described in Example III, we have reacted dimethyl acrylic acid ethyl ester with selenous acid added in small increments in the dry powder form. In this case the proportion of acid used was 30 grams to 50 grams of the dimethyl acrylic acid ethyl ester; otherwise the procedure was the same as in Example III and likewise the product obtained was the 'y-hydroxy-p-methyl crotonic acid ethyl ester.
Where herein we have referred to the esters or similar derivatives of the 11,,8 unsaturated aliphatic acids as being responsive to the indicated reactions, itwill be understood that the term similar derivatives is intended to include the corresponding anhydrides, acyl halogenides and nitriles, and that where in the claims the method is described as applied to the acids and their esters, the term esters is intended to include these similar derivatives.
Where in the claims reference is made to selenous acid as the reagent, it is to be understood that this term also includes selenium dioxide which is the functional equivalent for the purpose indicated.
Where in the claims reference is made to the crotonic acids it is to be understood that this term also includes the various substituted crotonic acids.
I claim:
1. The process for preparing 'y-hydroxy derivatives of normal and branched-chain oc-fi unsaturated aliphatic acid alkyl esters, which derivatives are characterized by the presence of an hydroxyl group in a methyl group attached to the B-carbon atom, which comprises reacting 2. The process for preparing 'y-hydroxy derivatives of normal and branched-chain oc-fl unsaturated aliphatic acid alkyl esters, which derivatives are characterized by the presence of an hydroxyl group in a methyl group attached to the c-carbon atom, which comprises reacting a member of the group consisting of the normal and branched-chain oc-fl unsaturated aliphatic acid alkyl esters having a methyl group attached to the B-carbon atom, with selenous acid in the presence of a solvent.
3. The process for preparing 'y-hydroxy derivatives of the methyl crotonic acid alkyl esters, which comprisesreacting a methyl crotonic acid alkyl ester with selenous acid.
4. The process for preparing hydroxy derivatives of the methyl crotonic acid alkyl esters, Which compries reacting a methyl crotonic acid alkyl ester with selenous acid in the presence of a solvent.
5. The process for preparing y-hYdIOXY-fimethyl crotonic acid ethyl ester which comprises reacting 5,5 dimethyl acrylic acid ethyl ester with selenous acid.
6. -hydroxy-c-methyl crotonic acid.
7. An alkyl ester of -hydroxy-p-methyl crotonic acid.
8. -hydroxy-c-methyl crotonic acid ethyl ester.
9. 'y-acetoxy-p-methyl crotonic acid ethyl ester.
10. A new compound of the general formula R.CHz.C.OHa
H.C.COOX
wherein R represents a radical selected from the group consisting of the acetoxy and hydroxyl groups, and wherein X represents a radical selected from the group consisting of hydrogen and an alkyl group.
HARRY H. SOBOTKA. MARTIN I. RUBIN.
Patent No. 2,590,555. CERTIFICAI'E- OF CORRECTION.
. December A, 1914.5;
HARRY H. SOBOTKA, ET AL- It is hereby oertified that error. appears in the printed specification of the above numbered patent requiring correction as follows: Page 1, sec-- 0nd column, line 59, for "2% hours" read "2% hours; and that the said Letters Patent should be read with this correction therein that the same. may conform to the reord of the case in the Patent Office.
Signed and sealed this 5th day of February, A. D. 1911.6.
Leslie Frazer (Sea1) First Assistant Commissioner of Patents.
US405408A 1941-08-04 1941-08-04 Method of preparing hydroxy derivatives of aliphatic acids and new compounds produced thereby Expired - Lifetime US2390335A (en)

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Cited By (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2459059A (en) * 1946-07-12 1949-01-11 Merck & Co Inc Method for preparing alkyl acyloxy acrylates
US2517588A (en) * 1946-11-12 1950-08-08 Samuel A Morell Process for manufacture of penaldic acids and their derivatives
US2752391A (en) * 1952-12-04 1956-06-26 Rohm & Haas Preparation of glyceric acid
US3879448A (en) * 1970-02-07 1975-04-22 Takeda Chemical Industries Ltd 4-hexenoic compounds

Cited By (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2459059A (en) * 1946-07-12 1949-01-11 Merck & Co Inc Method for preparing alkyl acyloxy acrylates
US2517588A (en) * 1946-11-12 1950-08-08 Samuel A Morell Process for manufacture of penaldic acids and their derivatives
US2752391A (en) * 1952-12-04 1956-06-26 Rohm & Haas Preparation of glyceric acid
US3879448A (en) * 1970-02-07 1975-04-22 Takeda Chemical Industries Ltd 4-hexenoic compounds

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